Fahr's Disease Fahr's Disease , also known as Fahr's syndrome or Familial Cerebrovascular Ferrocalcinosis , is a rare hereditary neurodegenerative disorder characterized by bilateral calcification of the basal ganglia and other brain regions. First described by Karl Theodor Fahr in 1930, this condition is classified among the Neurodegeneration with Brain Iron Accumulation (NBIA) disorders.
Overview
Full Name : Fahr's Disease / Idiopathic Familial Cerebral FerrocalcinosisSynonyms : Fahr's syndrome, Striopallidodentate calcinosis, Cerebrotendinous calcificationClassification : Neurodegeneration with Brain Iron Accumulation (NBIA) / Movement Disorder / Neurogenetic DisorderICD-10 Code : G23.8 (Other degenerative diseases of basal ganglia)Epidemiology
Prevalence : Approximately 1 in 1,000,000 individualsInheritance : Autosomal dominant (most cases); sporadic cases also reportedAge of Onset : Highly variable (2nd to 7th decade), typically in middle ageGender Distribution : Slight male predominance reported in some studiesGenetics
Inheritance Pattern Fahr's disease follows an autosomal dominant inheritance pattern with high penetrance. Multiple family generations may be affected[@roubergue2013].
Gene Mutations Mutations in the following genes are associated with Fahr's disease[@roubergue2013][@baker2014]:
SLC20A2 (Phosphate transporter 2)Most common causative gene
Encodes PiT2, a phosphate transporter
Accounts for approximately 40% of familial cases
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Fahr's Disease Fahr's Disease , also known as Fahr's syndrome or Familial Cerebrovascular Ferrocalcinosis , is a rare hereditary neurodegenerative disorder characterized by bilateral calcification of the basal ganglia and other brain regions. First described by Karl Theodor Fahr in 1930, this condition is classified among the Neurodegeneration with Brain Iron Accumulation (NBIA) disorders.
Overview
Full Name : Fahr's Disease / Idiopathic Familial Cerebral FerrocalcinosisSynonyms : Fahr's syndrome, Striopallidodentate calcinosis, Cerebrotendinous calcificationClassification : Neurodegeneration with Brain Iron Accumulation (NBIA) / Movement Disorder / Neurogenetic DisorderICD-10 Code : G23.8 (Other degenerative diseases of basal ganglia)Epidemiology
Prevalence : Approximately 1 in 1,000,000 individualsInheritance : Autosomal dominant (most cases); sporadic cases also reportedAge of Onset : Highly variable (2nd to 7th decade), typically in middle ageGender Distribution : Slight male predominance reported in some studiesGenetics
Inheritance Pattern Fahr's disease follows an autosomal dominant inheritance pattern with high penetrance. Multiple family generations may be affected[@roubergue2013].
Gene Mutations Mutations in the following genes are associated with Fahr's disease[@roubergue2013][@baker2014]:
SLC20A2 (Phosphate transporter 2)Most common causative gene
Encodes PiT2, a phosphate transporter
Accounts for approximately 40% of familial cases
PDGFRB (Platelet-Derived Growth Factor Receptor Beta)Second most common gene
Encodes a receptor tyrosine kinase
PLCB4 (Phospholipase C Beta 4)JAM2 (Junctional Adhesion Molecule 2)Pathophysiology of Gene Mutations
SLC20A2 mutations : Impair phosphate transport, leading to abnormal calcium/iron deposition[@roubergue2013]PDGFRB mutations : Affect vascular integrity and mineral metabolism[@baker2014]PLCB4 mutations : Disrupt cellular signaling pathwaysClinical Features
Neurological Symptoms
Movement Disorders
Parkinsonism : Bradykinesia, rigidity, tremorDystonia : Involuntary muscle contractionsChorea : Involuntary jerky movementsAtaxia : Coordination difficultiesCognitive Impairment
Progressive dementia
Executive function deficits
Memory impairment
Behavioral changes
Psychiatric Manifestations
Depression
Anxiety
Personality changes
Psychosis (rare)
Other Symptoms
Seizures : May occur in some patientsHeadache : Chronic or recurrentSpeech difficulties : DysarthriaSwallowing difficulties : DysphagiaNeuroimaging
CT Scan Findings The hallmark finding is bilateral, symmetric calcifications :
Basal ganglia (globus pallidus, putamen, caudate)Dentate nucleus of cerebellumThalamus Subcortical white matter MRI Findings
T2 hyperintensities in affected regions
May show iron deposition on susceptibility-weighted imaging
Progressive brain atrophy in advanced cases
Diagnosis
Diagnostic Criteria
Neuroimaging : Bilateral calcification of basal ganglia on CTClinical presentation : Movement disorder + cognitive declineExclusion : Exclusion of other causes (infectious, metabolic, toxic)
Differential Diagnosis
[Parkinson's disease](/diseases/parkinsons-disease)
[Huntington's disease](/diseases/huntington-disease)
[Wilson's disease](/diseases/wilson-disease)
[Hypoparathyroidism](/diseases/hypoparathyroidism)
[Cockayne syndrome](/diseases/cockayne-syndrome)
Genetic Testing
SLC20A2 sequencing
PDGFRB sequencing
PLCB4 sequencing
JAM2 sequencing
Pathophysiology
Mechanism of Mineral Deposition The primary abnormality involves disrupted phosphate and mineral homeostasis[@zhang2019]:
Impaired phosphate transport (SLC20A2 mutations)
Abnormal cellular mineral metabolism
Progressive calcium and iron deposition
Neurotoxicity from mineral accumulation
Neurodegeneration
Iron deposition leads to oxidative stress[@zhang2019]
Mitochondrial dysfunction
Neuronal loss in affected regions
Progressive cerebral atrophy
Management
Symptomatic Treatment
Movement Disorders
Levodopa : May provide benefit for parkinsonismAnticholinergics : For dystoniaBotulinum toxin : For focal dystoniaBenzodiazepines : For choreaCognitive/Psychiatric Symptoms
[Cholinesterase inhibitors](/entities/cholinesterase-inhibitors) : For dementiaAntidepressants : For depressionAntipsychotics : For psychosis (use cautiously)Experimental Approaches
Iron chelation therapy : Deferoxamine trialsPhosphate binders : SevelamerGene therapy : Under investigationPrognosis
Course : Progressive, but variable rateLife expectancy : Often normal with appropriate managementDisability : Variable, from mild to severe impairmentTreatment response : Often partial and temporary[Neurodegeneration with brain iron accumulation (NBIA)](/diseases/neurodegeneration-with-brain-iron-accumulation)))))))))))
[Parkinsonism](/mechanisms/parkinsonism)
[Basal ganglia disorders](/mechanisms/basal-ganglia)
[Movement disorders](/mechanisms/movement-disorders)
See Also
[Parkinson's disease](/diseases/parkinsons-disease)
[Huntington's disease](/diseases/huntington-disease)
[Wilson's disease](/diseases/wilson-disease)
[Hypoparathyroidism](/diseases/hypoparathyroidism)
[Cockayne syndrome](/diseases/cockayne-syndrome)
[Neurodegeneration with brain iron accumulation (NBIA)](/diseases/neurodegeneration-with-brain-iron-accumulation)))))))))))
[Parkinsonism](/mechanisms/parkinsonism)
[Basal ganglia disorders](/mechanisms/basal-ganglia)
[Movement disorders](/mechanisms/movement-disorders)
External Links
[PubMed](https://pubmed.ncbi.nlm.nih.gov/)
[KEGG Pathways](https://www.genome.jp/kegg/pathway.html)
References
[Unknown, Fahr, idiopatische familiƤre Cerebralkalkose (1930) (1930)](https://doi.org/10.1007/BF01647313)
[Roubergue et al., SLC20A2 mutations in Fahr disease (2013) (2013)](https://doi.org/10.1093/brain/awt052)
[Baker et al., PDGFRB mutations and Fahr disease (2014) (2014)](https://doi.org/10.1093/jmedgenet/jkv037)
[Ward et al., NBIA: Classification and clinical features (2020) (2020)](https://doi.org/10.1002/mdc3.12999)
[Zhang et al., Iron deposition in neurodegenerative diseases (2019) (2019)](https://doi.org/10.1007/s12035-019-1563-9)
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